Bispecific BCMA-CD3 Antibodies Block Multiple Myeloma Tumor Growth

抗体 多发性骨髓瘤 抗原 CD3型 细胞毒性T细胞 癌症研究 分子生物学 生物 免疫学 体外 CD8型 生物化学
作者
Lijun Wu,Yanwei Huang,John Sienkiewicz,Jinying Sun,Liselle Guiang,Feng Li,Liming Yang,Vita Golubovskaya
出处
期刊:Cancers [MDPI AG]
卷期号:14 (10): 2518-2518
标识
DOI:10.3390/cancers14102518
摘要

BCMA antigen is overexpressed in multiple myeloma cells and has been shown to be a promising target for novel cellular and antibody therapeutics. The humanized BCMA (clone 4C8A) antibody that effectively targeted multiple myeloma in a CAR (chimeric antigen receptor) format was used for designing several formats of bispecific BCMA-CD3 antibodies. Several different designs of univalent and bivalent humanized BCMA-CD3 CrossMAB and BCMA-FAB-CD3 ScFv-Fc antibodies were tested for binding with BCMA-positive cells and T cells and for killing by real time cytotoxic activity and IFN-gamma secretion with CHO-BCMA target cells and with multiple myeloma MM1S and H929 cell lines. All BCMA-CD3 antibodies demonstrated specific binding by FACS to CHO-BCMA, multiple myeloma cells, and to T cells with affinity Kd in the nM range. All antibodies with T cells specifically killed CHO-BCMA and multiple myeloma cells in a dose-dependent manner. The BCMA-CD3 antibodies with T cells secreted IFN-gamma with EC50 in the nM range. In addition, three BCMA bispecific antibodies had high in vivo efficacy using an MM1S xenograft NSG mouse model. The data demonstrate the high efficacy of novel hBCMA-CD3 antibodies with multiple myeloma cells and provide a basis for future pre-clinical and clinical development.
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